US 20060271168 A1
An implantable medical device is provided that degrades upon contact with body fluids so as to limit its residence time within the body. The device is formed of a porous corrodible metal to simultaneously provide high strength and an accelerated corrosion rate. The corrosion rate of a device formed of metal subject to self-dissolution or of a combination of metals subject to galvanic corrosion is accelerated by its porous structure. Coating the corrodible metallic device with a degradable polymer serves to delay the onset of corrosion of the underlying metallic structure.
1. An implantable, biodegradable medical device formed of a porous, corrodible metal.
2. The implantable medical device of
3. The implantable medical device of
4. The implantable medical device of
5. The implantable medical device of
6. The implantable medical device of
7. The implantable medical device of
8. The implantable medical device of
9. The implantable medical device of
10. The implantable medical device of
11. The implantable medical device of
12. An implantable stent formed of porous iron.
13. The implantable stent of
14. The scent of
15. The stent of
16. The stent of
17. An implantable stent, having a porous structure and formed of at least two metals, wherein said metals that form one or more internal galvanic couples.
18. The implantable stent of
19. The implantable stent of
20. The implantable stent of
21. The implantable stent of
This is a continuation-in-part of currently pending U.S. patent application Ser. No. 10/283,951, filed Oct. 30, 2002, entitled POROUS METAL FOR DRUG LOADED STENTS.
The present invention relates generally to medical devices which are adapted for implantation into a patient's body lumen and which are intended to degrade after implantation to eventually become absorbed and/or eliminated by the body. More particularly, the invention is applicable to a stent for deployment in a blood vessel in which its presence is only temporarily required.
Various medical devices are routinely implanted in a body lumen such as a blood vessel, wherein a permanent presence is not required and wherein an extended presence may actually be counterproductive. For example, stents are particularly useful in the treatment and repair of blood vessels after a stenosis has been compressed by percutaneous transluminal coronary angioplasty (PTCA), percutaneous transluminal angioplasty (PTA); or removed by atherectomy or other means, to help improve the results of the procedure and maintain patency. Alternatively, stents can be used to provide primary compression to a stenosis in cases in which no initial PTCA or PTA procedure is performed. It has however been found that the support that is provided by a stent is only required for a limited period of time, perhaps on the order of months, as the part of the vessel affected by stenosis would thereafter typically remain open even without any further support. The continued presence of some scent structures would then only serve as a permanent irritation of the tissue surrounding the stent, as the stent's rigidity could preclude it from performing the flexions caused by the heartbeat. An additional complication arises in pediatric applications because the stent comprises a fixed obstruction at the implantation site while such implantation site evolves with the growth of the child. Invasive retrieval of a stent is generally not considered to be a viable option.
While stents have typically been constructed of relatively inert metals in order to ensure their longevity, degradable stent structures have more recently been devised in an effort to provide support for only a limited period of time. Various polymeric substances are known that gradually dissolve and are absorbed by the body without adverse effect which has prompted the construction of stents with such polymers and polymer combinations for the purpose of providing only temporary support. It is however difficult to match the structural and mechanical properties of a metallic structure with the use of polymers, especially when polymeric materials are loaded with a drug, as drug loading of a polymeric material can have a significant adverse effect on strength. The need to minimize delivery profile as well as the desire to minimize bulk upon deployment substantially precludes simply increasing the dimensions of a polymeric stent in an effort to match the strength of a metallic structure.
It has more recently been found that certain metals, such as iron, are readily absorbable by the body without adverse effect. Consequently, the use of corrodible metals is being considered for use in degradable stent applications. Unfortunately, the corrosion rates of heretofore considered metallic structures have not been-sufficiently high so as to provide for as limited a residence time as may be desirable in certain applications. Simply reducing the dimensions of a metallic implantable medical device in order to reduce residence times may not be a viable option due the compromise in strength that necessarily results. An approach is therefore needed for accelerating the corrosion rate of a metallic structure without unacceptably compromising strength in order to limit the residence time of such device within the body. Moreover, it is most desirable to control the degradation of the device such that full strength is retained for a preselected period of time after which corrosion proceeds at an accelerated rate.
The present invention provides a degradable metallic medical device such as a stent which is configured to degrade at a sufficiently high rate so as to substantially limit its residence time within a body lumen in which it had been deployed. The device is formed of porous metal, wherein the metal is selected for its propensity to corrode upon contact with the bodily fluids in which it is immersed without adversely affecting the body, while the porosity is relied upon to increase the surface area in contact with such fluids and thereby accelerate the rate of its corrosion. By selecting the metal and the degree of porosity, rates of degradation can be tailored to a wide range of applications.
The metal selected for use in the construction of a medical device in accordance with the present invention may consist of a single element, such as iron, or may comprise a combination of metals. Generally, the metal(s) must be implantable without causing significant inflammation, neointimal proliferation or thrombotic events and must be corrodible so as to dissolve, dissociate or otherwise break down in the body without ill effect. “Degradable”, “biodegradable”, “biologically degradable”, “erodable”, “bioabsorbable ” and “bioresorbable” are all terms that have been used to describe this essential property.
In selecting a metal for practicing the present invention, it has been found that metals that form an oxide layer that grows and flakes off tend to corrode at appreciably higher rates than metals that form a contiguous oxide layer. Alternatively, the corrosion rate of a relatively slowly corroding metal can be accelerated by combining it with another metal selected so as to provide for a relatively high internal galvanic couple to yield a correspondingly high galvanic corrosion rate. As a further alternative, a metal can be selected for practicing the present invention based on its propensity to dissolve in vivo. Certain metals, including Mg for example, are subjected to a natural driving force of up to 50 mV when implanted in the body and are therefore subject to gradual dissolution.
Reliance on galvanic corrosion in order to achieve a desired corrosion rate requires the selection of a metal pair that has a sufficiently high rest potential differential. A rest potential differential results from two metals that, by themselves, each have a particular rest potential when measured versus a reference electrode, for example a Standard Calomel Electrode (SCE) or Natural Hydrogen Electrode (NHE), in the same type of solution, for example saline or equine horse serum. The driving force toward corrosion that results from this differential may be tailored to control the rate of degradation of the joined materials. For example, a driving force of about 500 mV would generally result in a slower dissolution than a driving force of 1 V or more. Appropriate metal pairs can be selected from among the elements Mg, Mn, K, Ca, Na, Zn, Cr, Fe, Cd, Al, Co, Sb, V, Cu and Mo, and from alloys based on such elements.
The degree of porosity that is imparted to the metal or combination of metals selected for use in the construction of the medical device is an essential element for the practice of the present invention. The porosity has a substantial effect on the rate of corrosion to the extent that the ratio of corrosion rate increase to surface area increase has been found to vary from 0.3 to 1.0 depending on the type of material and the environment to which it is exposed. The morphology of the microcellular porous metal, including the cell size and porosity of the metal, can be controlled so that the cell sizes can be made very uniform, and can be controlled precisely by the manipulation of various parameters during the formation process. The desired porosity is achievable by a variety of techniques including, but not limited to sintering, foaming, extrusion, thixomolding, semi-solid slurry casting and thermal spraying. The stent structure may be formed using any of the well known techniques, including, for example, the laser cutting of a tubular form.
The corrosion of the porous metallic medical device can additionally be modified with the application of a polymeric coating thereto. A coating with a degradable polymer serves to delay and/or reduce the corrosion of the underlying metal structure. For a fully degradable device, utilizing a degradable polymer, the performance of a coated device can be tailored so as to maintain up to its full structural strength for an initial period of time followed by more rapid degradation thereafter. The corrosion rates of selected portions of a medical device can additionally be differentiated with the application of either degradable and/or non-degradable polymeric coatings to only portions of the medical device.
The present invention additionally provides for the controlled release of therapeutic drugs by a degradable metallic medical device with the loading of such drugs directly into the pore structure of the device, or alternatively, with the loading of drugloaded polymers onto or into the porous medical device.
Other features and advantages of the present invention will become more apparent from the following detailed description when taken in conjunction with the accompanying exemplary drawings.
Catheter assembly 12 as depicted in
As shown in
In a typical procedure to implant stent 10, the guide wire 18 is advanced through the patient's vascular system by well known methods so that the distal end of the guide wire is advanced past the plaque or diseased area 25. Prior to implanting the stent, the cardiologist may wish to perform an angioplasty procedure or other procedure (e.g., atherectomy) in order to open the vessel and remodel the diseased area. Thereafter, the stent delivery catheter assembly 12 is advanced over the guide wire so that the stent is positioned in the target area. The expandable member or balloon 22 is inflated by well known means so that it expands radially outwardly and in turn expands the stent radially outwardly until the scent is apposed to the vessel wall. The expandable member is then deflated and the catheter withdrawn from the patient's vascular system. The guide wire typically is left in the lumen for post-dilatation procedures, if any, and subsequently is withdrawn from the patient's vascular system. As depicted in
The stent 10 serves to hold open the artery 24 after the catheter is withdrawn, as illustrated by
The stent patterns shown in
The stent illustrated in
Alternatively, the corrodible metal may comprise a combination of two or more metals selected to create a galvanic couple such that the material will undergo galvanic dissolution upon contact with bodily fluids. The degradation rate may be tailored by selecting a combination of metals that have a driving force of about 500 mV or greater. In a most preferred embodiment the driving force would be about 1 V or greater For example, Ti has a rest potential of 3.5 V vs. SCE in equine serum, and would, when paired with almost any other metal, yield a suitable driving force. Alternatively, the pairings Nb—Cr (1.1 V rest potential differential vs. SCE in equine serum), Pd—W (1.23 V rest potential vs. SCE in equine serum) and Cr—W (630 mV rest potential differential vs. SCE in equine serum) would also yield suitable driving forces.
Any of a variety of well-known manufacturing techniques can be relied upon to achieve a sufficient degree of porosity in the metallic structure be it a single element such as iron or a Nb—Cr pairing. Such techniques include but are not limited to sintering, extrusion, thixomolding, semi-solid casting and thermal spraying. A preferred method comprises the formation of microcellular metallic foams as developed at Massachusetts Institute of Technology and Clarkson University, as outlined in V. Kumar and N. P. Sub, Polym. Eng. Sci., 30, pp. 1323-1329(1990), and C. Wang, K. Cox and G. Campbell, J. Vinyl Additives Tech., 2(2), pp. 167-169(1996). Such microcellular foams are typically characterized by cell sizes or diameters in the range of 0.1 to 100 microns, and cell densities in the range of 109 to 1015 cells per cubic cm. The foaming process can be carried out on metallic preforms such as extruded hypotubing of a desired dimension. The first stage of microcellular foam processing involves dissolving an inert gas, such as nitrogen or CO2, under pressure into the metallic matrix. The next phase is the rapid creation of microvoids. This is initiated by inducing large thermodynamic instability by quickly decreasing the solubility of the gas in the metal b y changing the pressure or temperature. Other various techniques known in the art can be used to fabricate microcellular porous metal. For example, microcellular porous metal carf be fabricated by employing the technique of powder technology which involves mixing a select polymer with metal powder and using an injection molding process to shape the tube or the stent preform. Alternatively, an electrolytic process for the deposition of a metal onto a polymer foam precursor by way of electrolytic deposition can be used to fabricate porous metal. The morphology of the microcellular porous metal, including the cell size and porosity of the metal, can be controlled so that the cell sizes can be made very uniform, and can be controlled precisely by changing thermodynamic variables like pressure and temperature during formation of the microcellular porous metal. The microcellular porous metal can be formed by a batch process that can be easily controlled and operated, in which extruded tubing can be cut to the desired lengths and then foamed in a separate pressure chamber.
After a tube of porous metal has been formed, a stent as illustrated in the Figures is manufactured by for example laser cutting the tube so as to remove material and leave portions of the metallic tubing which are to form the rings, struts and links. In accordance with the invention, it is preferred to cut the tubing in the desired pattern using a machine-controlled laser which process is well known in the art. After laser cutting, the stent rings are subjected to a surface smoothing mechanism such as bead blasting with a safe media, honing, etc. Electropolishing is also an option, although the solution used must be selected so as to minimize degradation, an example of which is ELECTRO-GLO #300, sold by the ELECTRO-GLO Co., Inc. in Chicago, Ill., which is a mixture of sulfuric acid, carboxylic acids, phosphates, corrosion inhibitors and a biodegradable surface active agent. The bath temperature, current density and cathode to anode area are selected according to principles well known in the art.
A bioabsorbable polymer coating may additionally be applied about the exterior of the porous structure in order to delay the corrosion process of the underlying metallic structure. Suitable polymers include but are not limited to polyalkanoates (PHA), poly(3-hydroxyalkanoates), such as poly(3-hydroxypropanoate), poly(3-hydroxybutyrate) (PHB), poly(3-hydroxyvalerate) (PHV), poly(3-hydroxybutyrate-co-3-hydroxyvalerate) (PHBV), poly(3-hydroxyhexanoate), poly(3-hydroxyheppanoate) and poly(3-hydroxyoctanoate), poly(4-hydroxyalkanoate) such as poly(4-hydroxybutyrate), poly(4-hydroxyvalerate), poly(4-hydroxyhexanoate), poly(4-hydroxyheptanoate), poly(4-hydroxyoctanoate) and copolymers comprising any of the 3-hydroxyalkanoate or 4-hydroxyalkanoate monomers described herein or blends thereof, polyesters, poly(DL-lactide), poly(L-lactide), polyglycolide, poly(lactide-co-glycolide), polycaprolactone, poly(lactide-co-caprolactone), poly(glydolide-co-caprolactone), poly(dioxanone), poly(ortho esters), poly(anhydrides), poly(tyrosine carbonates) and derivatives thereof, poly(tyrosine ester) and derivatives thereof, poly(imino carbonates), poly(phosphoesters), poly(phosphazenes), poly(amino acids), polysaccharides, collagen, chitosan, alginate, and PolyAspirin.
Stents relying on a self-dissolving metal to achieve an accelerated degradation rate in accordance with the present invention may be formed of Mg, Mn, K, Ca, Na, Zn, Cr, Fe, Cd, Al, Co, Sb, V, Cu and Mo, or alloys thereof. More preferably, such stents are formed of K, Na, Mg, Zn, Cd, Al, In and Fe and most preferably of K, Na, Mg, Zn and Fe or alloys thereof. Stents relying on galvanic corrosion to achieve an accelerated degradation rate in accordance with the present invention are preferably formed of element or alloy combinations with at least about 500 mV of driving force, more preferably with at least about 800 mV of driving force and most preferably with at least about 1 V of driving force. The porosity of the metal structure of such stents is preferably at least about 10%, more preferably 30% - 80% and most preferably 40% - 60%.
While the invention has been described in connection with certain disclosed embodiments, it is not intended to limit the scope of the invention to the particular forms set forth, but, on the contrary it is intended to cover all such alternatives, modifications, and equivalents as may be included in the spirit and scope of the invention as defined by the appended claims.